Diadenosine tetraphosphate or Ap4A is a putative alarmone, ubiquitous in nature being common to everything from bacteria to humans. It is made up of two adenosines joined together by a 5′-5′ linked chain of four phosphates. Adenosine polyphosphates are capable of inducing multiple physiological effects.[1]
Function
In Eukaryotes
Ap4A can be created by a non-canonical activity of the Lysyl-tRNA synthetase (LysRS). This function of LysRS is activated by the phosphorylation of LysRS on serine 207, its subsequent dissociation from the multi-synthetase complex (MSC).[2] The molecule's role as a second messenger has recently been discovered in The LysRS-Ap4A-MITF signaling pathway.[3] Ap4A binds to the MITF-HINT1 inhibitory complex, specifically to the molecule histidine triad nucleotide–binding protein 1(HINT1), releasing the Microphthalmia-associated transcription factor (MITF) and causing an increase in the transcription of its target genes.[4] Ap4A also positively regulates the activity of the transcription factor USF2 through a similar molecular mechanism to that of MITF.[5]
It has also been shown, that Ap4A plays a role in the functionality of dendritic cells (DCs). An increase in the intracellular amount Improves their motility and antigen presenting ability through alterations in small GTPases present in the cells. This was discovered by creating mice deficient in the enzyme NUDT2, which serves as an Ap4A hydrolase and thus controls the levels of Ap4A in the cell.[6] Ap4A, however, has also been shown to cause apoptosis in several cell lines through an unknown mechanism, the degradation of Ap4A was necessary for the process as hydrolysis-resistant analogues of the molecule showed no apoptotic activity.[7]
In Prokaryotes
In E. Coli, Ap4A has been shown to function as an alarmone, as the intracellular concentration of the molecule increases upon heat stress.[8] Ap4A can also be incorporated into RNA as a 5' Cap along with other dinucleoside polyphosphates. It serves as a substrate for the RNA polymerase and the intracellular levels of these capped RNAs increase upon stress, suggesting that the cap adds a level of stability to the RNA.[9]
Myxococcus xanthus is a type of Gram-negative bacteria, and M. xanthus lysyl-tRNA synthetase (LysS) is an enzyme from the bacteria that synthesizes diadenosine tetraphosphates (Ap4A) when adenosine triphosphate (ATP) is present. Diadenosine pentaphosphate (Ap5A) is synthesized from Ap4A with ATP.[10]
References
^Luo, Jiankai; Jankowski, Vera; GüNgär, Nihayrt; Neumann, Joachim; Schmitz, Wilhelm; Zidek, Walter; SchlüTer, Hartmut; Jankowski, Joachim (2004). "Endogenous diadenosine tetraphosphate, diadenosine pentaphosphate, and diadenosine hexaphosphate in human myocardial tissue". Hypertension. 43 (5): 1055–9. doi:10.1161/01.hyp.0000126110.46402.dd. PMID15066958. S2CID1003539.
^*Lee, Yu-Nee; Nechushtan, Hovav; Figov, Navah; Razin, Ehud (April 2004). "The function of lysyl-tRNA synthetase and Ap4A as signaling regulators of MITF activity in FcepsilonRI-activated mast cells". Immunity. 20 (2): 145–51. doi:10.1016/S1074-7613(04)00020-2. PMID14975237. S2CID36723485.
^Kimura, Yoshio; Tanaka, Chihiro; Oka, Manami (July 2018). "Identification of Major Enzymes Involved in the Synthesis of Diadenosine Tetraphosphate and/or Adenosine Tetraphosphate in Myxococcus xanthus". Current Microbiology. 75 (7): 811–817. doi:10.1007/s00284-018-1452-x. ISSN1432-0991. PMID29468302. S2CID3402370.